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Discovery of hepatitis B virus capsid assembly inhibitors leading to a heteroaryldihydropyrimidine based clinical candidate (GLS4)

机译:发现乙型肝炎病毒衣壳组装抑制剂,导致杂芳基吡啶基酰亚胺基于临床候选者(GLS4)

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Inhibition of hepatitis B virus (HBV) capsid assembly is a novel strategy for the development of chronic hepatitis B (CHB) therapeutics. Herein we described our lead optimization studies including the synthesis, molecular docking studies and structure-activity relationship (SAR) studies of a series of novel heteroaryldihydropyrimidine (HAP) inhibitors of HBV capsid assembly inhibitors, and the discovery of a potent inhibitor of HBV capsid assembly of GLS4 (ethyl 4-[2-bromo-4-fluoropheny1]-6-[morpholinomethy1]-242-thiazoly1]-1,4-dihydro-pyrimidine-5-carboxylate) which is now in clinical phase 2. GLS4 demonstrated potent inhibitory activities in HBV HepG2.2.15 cell assay with an EC50 value of 1 nM, and it also exhibited high potency against various drug-resistant HBV viral strains with EC50 values in the range of 10-20 nM, more potent than the typical HBV polymerase inhibitors such as lamivudine, telbivudine, and entecavir. Pharmacokinetic profiles of GLS4 were favorable and safety evaluation including acute toxicity and repeated toxicity study indicated that GLS4 was safe enough to support clinical experiments in human. (C) 2016 Elsevier Ltd. All rights reserved.
机译:乙型肝炎病毒(HBV)胶囊组装的抑制是一种新型慢性乙型肝炎(CHB)治疗剂的策略。在此,我们描述了我们的铅优化研究,包括合成,分子对接研究和结构 - 活性关系(SAR)研究HBV胶囊组装抑制剂的一系列新型杂芳基吡啶啉烷(HAP)抑制剂,以及HBV胶囊组装的有效抑制剂的发现GLS4(乙基4- [2-溴-4-氟苯键1] -6- [morpholinomethy1] -242-吡啶胺-5-羧酸盐),其目前在临床阶段2. GLS4表现出有效的HBV HepG2.2.15中的抑制活性在EC50值为1nm的细胞测定中,它还表现出对各种耐药性HBV病毒菌株的高效力,其EC50值在10-20nm的范围内,比典型的HBV聚合酶更有效抑制剂如拉米夫定,左侧诱导和埃内斯切韦。 GLS4的药代动力学谱是有利的,并且在包括急性毒性和反复毒性研究的安全评估表明GLS4足以支持人类的临床实验。 (c)2016 Elsevier Ltd.保留所有权利。

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